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登革病毒感染的自体单核细胞诱导人淋巴细胞产生α干扰素。

Induction of interferon alpha from human lymphocytes by autologous, dengue virus-infected monocytes.

作者信息

Kurane I, Ennis F A

机构信息

Department of Medicine, University of Massachusetts Medical Center, Worcester 01605.

出版信息

J Exp Med. 1987 Oct 1;166(4):999-1010. doi: 10.1084/jem.166.4.999.

Abstract

Human monocytes actively replicate dengue virus. To dissect the primary immune responses to dengue virus-infected monocytes (DV-monocytes), we analyzed the interaction between autologous DV-monocytes and the peripheral blood lymphocytes (PBL) of dengue nonimmune donors. Interferon (IFN) activity was detected when PBL were cultured with DV-monocytes. Cell contact between PBL and DV-monocytes was required for IFN production; however, MHC compatibility between PBL and monocytes was not necessary. DV-monocytes fixed with paraformaldehyde or glutaraldehyde, which produced no infectious virus, also induced high levels of IFN from PBL. The ability of DV-monocytes to induce IFN correlated with the appearance of dengue antigens. The PBL that produce IFN were characterized by FACS sorting using monoclonal and polyclonal antibodies. HLA-DR+ and T3- cells produced high titers of IFN, while HLA-DR- and T3+ cells produced very low or undetectable levels of IFN. Moderate titers of IFN were produced by cells contained in B cell fractions (surface immunoglobulin-positive, B1+, and Leu-12+), and cells contained in natural killer cell fractions (Leu-11+ and OKM1+). Therefore, IFN-producing cells are heterogeneous, and the predominant producer cells are characterized as HLA-DR+ and non-T lymphocytes. The IFN produced was characterized by RIA using mAbs to IFN-alpha and IFN-gamma. The IFN-alpha was the predominant IFN produced; in addition, a low level of IFN-gamma was also detected in some experiments. The culture fluids obtained from PBL exposed to autologous DV-monocytes, which contained high IFN activity, completely inhibited dengue virus infection of monocytes. These results suggest that IFN-alpha produced by PBL exposed to DV-monocytes may play an important role in controlling primary dengue virus infection.

摘要

人类单核细胞可活跃地复制登革病毒。为剖析对登革病毒感染的单核细胞(DV - 单核细胞)的初始免疫反应,我们分析了自体DV - 单核细胞与登革热非免疫供体的外周血淋巴细胞(PBL)之间的相互作用。当PBL与DV - 单核细胞共培养时可检测到干扰素(IFN)活性。IFN产生需要PBL与DV - 单核细胞之间的细胞接触;然而,PBL与单核细胞之间的MHC相容性并非必需。用多聚甲醛或戊二醛固定的不产生感染性病毒的DV - 单核细胞,也能诱导PBL产生高水平的IFN。DV - 单核细胞诱导IFN的能力与登革热抗原的出现相关。通过使用单克隆和多克隆抗体的FACS分选对产生IFN的PBL进行了表征。HLA - DR⁺和T3⁻细胞产生高滴度的IFN,而HLA - DR⁻和T3⁺细胞产生的IFN水平非常低或无法检测到。B细胞组分(表面免疫球蛋白阳性、B1⁺和Leu - 12⁺)中的细胞以及自然杀伤细胞组分(Leu - 11⁺和OKM1⁺)中的细胞产生中等滴度的IFN。因此,产生IFN的细胞是异质性的,主要的产生细胞被表征为HLA - DR⁺和非T淋巴细胞。使用针对IFN - α和IFN - γ的单克隆抗体通过放射免疫分析(RIA)对产生的IFN进行了表征。IFN - α是产生的主要IFN;此外,在一些实验中也检测到了低水平的IFN - γ。从暴露于自体DV - 单核细胞的PBL获得的含有高IFN活性的培养液,完全抑制了单核细胞的登革病毒感染。这些结果表明,暴露于DV - 单核细胞的PBL产生的IFN - α可能在控制登革病毒的初始感染中起重要作用。

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本文引用的文献

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MESSENGER RNA FOR INTERFERON PRODUCTION.
Proc Soc Exp Biol Med. 1965 Feb;118:384-5. doi: 10.3181/00379727-118-29850.
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